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首页> 外文期刊>Hepatology: Official Journal of the American Association for the Study of Liver Diseases >Clinical cofactors and hepatic fibrosis in hereditary hemochromatosis: The role of diabetes mellitus
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Clinical cofactors and hepatic fibrosis in hereditary hemochromatosis: The role of diabetes mellitus

机译:遗传性血色素沉着症中的临床辅助因子和肝纤维化:糖尿病的作用

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The risk of hepatic fibrosis and cirrhosis in hereditary hemochromatosis relates to the degree of iron loading, but iron alone does not explain the variability in disease penetrance. This study sought to identify clinical cofactors that increase the risk of progressive liver disease. We identified 291 patients from our database who were homozygous for the C282Y mutation in HFE and had undergone a liver biopsy with quantification of hepatic iron concentration (HIC) and fibrosis staging. Data were collected from a retrospective chart review, including age, gender, alcohol consumption, medical therapy, smoking history, metabolic risk factors, mobilizable iron, and laboratory results. Male gender, excess alcohol consumption, HIC, and the presence of diabetes were independently associated with increasing fibrosis stage in multivariate analysis. Of these, the presence of diabetes showed the strongest association (odds ratio, 7.32; P = 0.03). The presence of steatosis was associated with higher fibrosis scores, but this was of borderline statistical significance. Risk factors for hepatic steatosis were male gender, impaired glucose tolerance, and increased body mass index. Conclusion: The presence of diabetes was associated with more severe hepatic fibrosis independent of iron loading, male gender, and alcohol consumption. The mechanism for this association is unknown and deserves further evaluation; however, it is possible that diabetes produces an additional hepatic oxidative injury from hyperglycemia. Thus, management of such cofactors in patients with hemochromatosis is important to reduce the risk of liver injury and fibrosis.
机译:遗传性血色素沉着病的肝纤维化和肝硬化的风险与铁负荷的程度有关,但仅铁并不能解释疾病pen愈的变异性。这项研究试图确定增加进行性肝病风险的临床辅助因子。我们从数据库中鉴定出291例患者,这些患者是HFE中C282Y突变的纯合子,并接受了肝活检,并定量了肝铁浓度(HIC)和纤维化分期。从回顾性图表审查中收集数据,包括年龄,性别,饮酒,药物治疗,吸烟史,代谢风险因素,可动铁和实验室检查结果。在多变量分析中,男性,过量饮酒,HIC和糖尿病的存在与纤维化阶段的增加独立相关。其中,糖尿病的存在显示出最强的关联性(优势比为7.32; P = 0.03)。脂肪变性的存在与较高的纤维化评分相关,但这具有临界的统计学意义。肝脂肪变性的危险因素是男性,糖耐量减低和体重指数增加。结论:糖尿病的存在与更严重的肝纤维化有关,而与铁负荷,男性和饮酒无关。这种关联的机制尚不清楚,值得进一步评估。但是,糖尿病可能会因高血糖症而产生额外的肝氧化损伤。因此,在血色素沉着病患者中管理此类辅助因子对于降低肝损伤和纤维化的风险很重要。

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